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一种优化的竞争性衰老方法揭示了……时序寿命背后的基因-药物相互作用。 (原文句末不完整)

An Optimized Competitive-Aging Method Reveals Gene-Drug Interactions Underlying the Chronological Lifespan of .

作者信息

Avelar-Rivas J Abraham, Munguía-Figueroa Michelle, Juárez-Reyes Alejandro, Garay Erika, Campos Sergio E, Shoresh Noam, DeLuna Alexander

机构信息

Unidad de Genómica Avanzada (Langebio), Centro de Investigación y de Estudios Avanzados del IPN, Irapuato, Mexico.

Broad Institute of MIT and Harvard, Cambridge, MA, United States.

出版信息

Front Genet. 2020 May 14;11:468. doi: 10.3389/fgene.2020.00468. eCollection 2020.

Abstract

The chronological lifespan of budding yeast is a model of aging and age-related diseases. This paradigm has recently allowed genome-wide screening of genetic factors underlying post-mitotic viability in a simple unicellular system, which underscores its potential to provide a comprehensive view of the aging process. However, results from different large-scale studies show little overlap and typically lack quantitative resolution to derive interactions among different aging factors. We previously introduced a sensitive, parallelizable approach to measure the chronological-lifespan effects of gene deletions based on the competitive aging of fluorescence-labeled strains. Here, we present a thorough description of the method, including an improved multiple-regression model to estimate the association between death rates and fluorescent signals, which accounts for possible differences in growth rate and experimental batch effects. We illustrate the experimental procedure-from data acquisition to calculation of relative survivorship-for ten deletion strains with known lifespan phenotypes, which is achieved with high technical replicability. We apply our method to screen for gene-drug interactions in an array of yeast deletion strains, which reveals a functional link between protein glycosylation and lifespan extension by metformin. Competitive-aging screening coupled to multiple-regression modeling provides a powerful, straight-forward way to identify aging factors in yeast and their interactions with pharmacological interventions.

摘要

出芽酵母的时序寿命是衰老及与年龄相关疾病的一种模型。这种范例最近使得在一个简单的单细胞系统中对有丝分裂后生存能力的潜在遗传因素进行全基因组筛选成为可能,这突出了其提供衰老过程全面视图的潜力。然而,不同大规模研究的结果显示出很少的重叠,并且通常缺乏定量分辨率来推导不同衰老因素之间的相互作用。我们之前引入了一种基于荧光标记菌株的竞争性衰老来测量基因缺失对时序寿命影响的灵敏、可并行化方法。在此,我们对该方法进行了详尽描述,包括一种改进的多元回归模型,用于估计死亡率与荧光信号之间的关联,该模型考虑了生长速率和实验批次效应中可能存在的差异。我们展示了针对十种具有已知寿命表型的缺失菌株,从数据采集到相对存活率计算的实验过程,该过程具有很高的技术可重复性。我们应用我们的方法在一系列酵母缺失菌株中筛选基因 - 药物相互作用,这揭示了蛋白质糖基化与二甲双胍延长寿命之间的功能联系。竞争性衰老筛选与多元回归建模相结合,为鉴定酵母中的衰老因素及其与药物干预的相互作用提供了一种强大且直接的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8484/7240105/b5e8e9428625/fgene-11-00468-g001.jpg

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